Abstract
Genes are transcribed in a discontinuous pattern referred to as RNA bursting, but the mechanisms regulating this process are unclear. Although many physiological signals, including glucocorticoid hormones, are pulsatile, the effects of transient stimulation on bursting are unknown. Here we characterize RNA synthesis from single-copy glucocorticoid receptor (GR)-regulated transcription sites (TSs) under pulsed (ultradian) and constant hormone stimulation. In contrast to constant stimulation, pulsed stimulation induces restricted bursting centered around the hormonal pulse. Moreover, we demonstrate that transcription factor (TF) nuclear mobility determines burst duration, whereas its bound fraction determines burst frequency. Using 3D tracking of TSs, we directly correlate TF binding and RNA synthesis at a specific promoter. Finally, we uncover a striking co-bursting pattern between TSs located at proximal and distal positions in the nucleus. Together, our data reveal a dynamic interplay between TF mobility and RNA bursting that is responsive to stimuli strength, type, modality, and duration. Stavreva et al. reveal a delay between glucocorticoid receptor (GR) binding and RNA synthesis and link GR mobility modulations in time- and treatment-dependent manner to the size and frequency of transcriptional bursts based on single molecule experiments. By reconstructing GR signaling dynamics on timescales ranging from days to milliseconds, they relate single-cell and single-molecule phenomena to glucocorticoid physiology.
| Original language | American English |
|---|---|
| Pages (from-to) | 1161-1177.e11 |
| Journal | Molecular Cell |
| Volume | 75 |
| Issue number | 6 |
| DOIs | |
| State | Published - 19 Sep 2019 |
Keywords
- 3D orbital tracking
- RNA synthesis
- bursting kinetics
- circadian cycle
- glucocorticoid receptor
- high-throughput imaging
- single cell
- single molecule tracking
- transcription dynamics
- ultradian hormone stimulation
EGS Disciplines
- Physics